journal
https://read.qxmd.com/read/38416029/granzyme-f-exhaustion-marker-and-modulator-of-chimeric-antigen-receptor-t-cell-mediated-cytotoxicity
#41
JOURNAL ARTICLE
Zachary L Z Hay, Dale D Kim, Jennifer M Cimons, Jennifer R Knapp, M Eric Kohler, Mary Quansah, Tiffany M Zúñiga, Faye A Camp, Mayumi Fujita, Xiao-Jing Wang, Brian P O'Connor, Jill E Slansky
Granzymes are a family of proteases used by CD8 T cells to mediate cytotoxicity and other less-defined activities. The substrate and mechanism of action of many granzymes are unknown, although they diverge among the family members. In this study, we show that mouse CD8+ tumor-infiltrating lymphocytes (TILs) express a unique array of granzymes relative to CD8 T cells outside the tumor microenvironment in multiple tumor models. Granzyme F was one of the most highly upregulated genes in TILs and was exclusively detected in PD1/TIM3 double-positive CD8 TILs...
February 28, 2024: Journal of Immunology
https://read.qxmd.com/read/38416013/retraction-ku86-variant-expression-and-function-in-multiple-myeloma-cells-is-associated-with-increased-sensitivity-to-dna-damage
#42
Yu-Tzu Tai, Gerrard Teoh, Boris Lin, Faith E Davies, Dharminder Chauhan, Steven P Treon, Noopur Raje, Teru Hideshima, Yoshihito Shima, Klaus Podar, Kenneth C Anderson
We wish to retract the article titled "Ku86 Variant Expression and Function in Multiple Myeloma Cells Is Associated with Increased Sensitivity to DNA Damage" by Yu-Tzu Tai, Gerrard Teoh, Boris Lin, Faith E. Davies, Dharminder Chauhan, Steven P. Treon, Noopur Raje, Teru Hideshima, Yoshihito Shima, Klaus Podar, and Kenneth C. Anderson, The Journal of Immunology, 2000, 165:6347-6355. There are concerns about the reliability of certain data, arising from errors in the assembly of Figs. 1B, 1D. The authors have concluded that these figures cannot be used to support the conclusions of the article...
February 28, 2024: Journal of Immunology
https://read.qxmd.com/read/38407485/induction-of-mthfd2-in-macrophages-inhibits-reactive-oxygen-species-mediated-nf-%C3%AE%C2%BAb-activation-and-protects-against-inflammatory-responses
#43
JOURNAL ARTICLE
Yan Cui, Zihan Li, Lina Ni, Sujun Yu, Xiao Shan, Penghui Hu, Zemin Ji, Weijia Jing, Yanzhao Zhou, Baochen Wang, Hongyuan Dong, Jinxue Zhou, Keliang Xie, Qiujing Yu
The one-carbon metabolism enzyme methylenetetrahydrofolate dehydrogenase 2 (MTHFD2) is critical for cancer cell proliferation and immune cell phenotypes, but whether it can contribute to macrophage inflammatory responses remains unclear. In this study, we show that MTHFD2 was upregulated by LPS in murine macrophages upon activation of the TLR4-MyD88-IKKα/β-NF-κB signaling pathway. MTHFD2 significantly attenuated LPS-induced macrophage proinflammatory cytokine production through its enzymatic activity...
February 26, 2024: Journal of Immunology
https://read.qxmd.com/read/38407351/correction-myeloid-heterogeneity-mediates-acute-exacerbations-of-pulmonary-fibrosis
#44
Jennifer L Larson-Casey, Komal Saleem, Ranu Surolia, Jyotsana Pandey, Matthias Mack, Veena B Antony, Sandeep Bodduluri, Surya P Bhatt, Steven R Duncan, A Brent Carter
We thank Denise Stanford and the UAB Cystic Fibrosis Research Center Assay Core (The University of Alabama at Birmingham, Birmingham, AL) for assistance with microCT acquisition and image processing. Additional support was provided by the UAB Research and Development Program from the Cystic Fibrosis Foundation (Grant ROWE19RO [DAVIS]).
February 26, 2024: Journal of Immunology
https://read.qxmd.com/read/38391367/trypanosoma-brucei-invariant-surface-glycoprotein-75-is-an-immunoglobulin-fc-receptor-inhibiting-complement-activation-and-antibody-mediated-cellular-phagocytosis
#45
JOURNAL ARTICLE
Jakob Hauge Mikkelsen, Kristian Stødkilde, Maria Pauladòttir Jensen, Annette Gudmann Hansen, Qi Wu, Josefine Lorentzen, Jonas Heilskov Graversen, Gregers Rom Andersen, Robert Andrew Fenton, Anders Etzerodt, Steffen Thiel, Christian Brix Folsted Andersen
Various subspecies of the unicellular parasite Trypanosoma brucei cause sleeping sickness, a neglected tropical disease affecting millions of individuals and domestic animals. Immune evasion mechanisms play a pivotal role in parasite survival within the host and enable the parasite to establish a chronic infection. In particular, the rapid switching of variant surface glycoproteins covering a large proportion of the parasite's surface enables the parasite to avoid clearance by the adaptive immune system of the host...
February 23, 2024: Journal of Immunology
https://read.qxmd.com/read/38391298/astaxanthin-inhibits-sting-carbonylation-and-enhances-antiviral-responses
#46
JOURNAL ARTICLE
Qizhao Li, Mutian Jia, Hui Song, Jun Peng, Wei Zhao, Weifang Zhang
STING-mediated DNA sensing pathway plays a crucial role in the innate antiviral immune responses. Clarifying its regulatory mechanism and searching STING agonists has potential clinical implications. Although multiple STING agonists have been developed to target cancer, there are few for the treatment of infectious diseases. Astaxanthin, a natural and powerful antioxidant, serves many biological functions and as a potential candidate drug for many diseases. However, how astaxanthin combats viruses and whether astaxanthin regulates the cyclic GMP-AMP synthase-STING pathway remains unclear...
February 23, 2024: Journal of Immunology
https://read.qxmd.com/read/38391297/ido1-inhibition-promotes-activation-of-tumor-intrinsic-stat3-pathway-and-induces-adverse-tumor-protective-effects
#47
JOURNAL ARTICLE
Longbo Yu, Lingyan Xu, Yunjie Chen, Yicheng Rong, Yi Zou, Shushan Ge, Tiancong Wu, Yisheng Lai, Qiang Xu, Wenjie Guo, Wen Liu
Pharmacological inhibition of IDO1 exhibits great promise as a strategy in cancer therapy. However, the failure of phase III clinical trials has raised the pressing need to understand the underlying reasons for this outcome. To gain comprehensive insights into the reasons behind the clinical failure of IDO1 inhibitors, it is essential to investigate the entire tumor microenvironment rather than focusing solely on individual cells or relying on knockout techniques. In this study, we conducted single-cell RNA sequencing to determine the overall response to apo-IDO1 inhibitor administration...
February 23, 2024: Journal of Immunology
https://read.qxmd.com/read/38381001/il-33-induces-cellular-and-exosomal-mir-146a-expression-as-a-feedback-inhibitor-of-mast-cell-function
#48
JOURNAL ARTICLE
Marcela T Taruselli, Amina Abdul Qayum, Daniel Abebayehu, Heather L Caslin, Jordan M Dailey, Aditya Kotha, Jason R Burchett, Sydney A Kee, Tania D Maldonado, Boyang Ren, Wei Chao, Lin Zou, Tamara T Haque, David Straus, John J Ryan
IL-33 is an inflammatory cytokine that promotes allergic disease by activating group 2 innate lymphoid cells, Th2 cells, and mast cells. IL-33 is increased in asthmatics, and its blockade suppresses asthma-like inflammation in mouse models. Homeostatic control of IL-33 signaling is poorly understood. Because the IL-33 receptor, ST2, acts via cascades used by the TLR family, similar feedback mechanisms may exist. MicroRNA (miR)-146a is induced by LPS-mediated TLR4 signaling and serves as a feedback inhibitor...
February 21, 2024: Journal of Immunology
https://read.qxmd.com/read/38380993/fosl2-deficiency-predisposes-mice-to-osteopetrosis-leading-to-bone-marrow-failure
#49
JOURNAL ARTICLE
Jinfeng Chen, Yi Wen, Lili Lin, Yuchen Cui, Zhenyu Chen, Jing Gao, Yifang Zhuang, Qi Chen
Arthritis causes Fos-like 2 (Fosl2) inactivation, and various immune cells contribute to its pathogenesis. However, little is known about the role of Fosl2 in hematopoiesis and the possible pathological role of Fosl2 inactivation in the hematopoietic system in arthritis. In this study, we show that Fosl2 maintains hematopoietic stem cell (HSC) quiescence and differentiation while controlling the inflammatory response via macrophages. Fosl2-specific deletion in the hematopoietic system caused the expansion of HSCs and myeloid cell growth while affecting erythroid and B cell differentiation...
February 21, 2024: Journal of Immunology
https://read.qxmd.com/read/38380986/the-role-of-fc-receptors-in-the-innate-immune-system-of-flounders-purported-to-be-homologs-of-fc%C3%AE-rii-and-fc%C3%AE-riii
#50
JOURNAL ARTICLE
Yan-Bo Hao, Jing Xing, Xiu-Zhen Sheng, Heng Chi, Xiao-Qian Tang, Wen-Bin Zhan
FcγR is a significant opsonin receptor located on the surface of immune cells, playing a crucial role in Ab-dependent cell-mediated immunity. Our previous work revealed opposite expression trends of FcγRII and FcγRIII in flounder mIgM+ B lymphocytes after phagocytosis of antiserum-opsonized Edwardsiella tarda. This observation suggests that FcγRII and FcγRIII might serve distinct functions in Ig-opsonized immune responses. In this study, we prepared rFcγRIII as well as its corresponding Abs to investigate the potential roles of FcγRII and FcγRIII in the Ab-dependent immune response of IgM+ B cells...
February 21, 2024: Journal of Immunology
https://read.qxmd.com/read/38372645/critical-role-of-cd55-in-controlling-wound-healing
#51
JOURNAL ARTICLE
Lorna Kang, Maryo Kohen, Isaac McCarthy, Emma Hammelef, Hae Suk Kim, R Bapputty, Rose Gubitosi-Klug, Faruk H Orge, Timothy Kern, M Edward Medof
How reparative processes are coordinated following injury is incompletely understood. In recent studies, we showed that autocrine C3a and C5a receptor (C3ar1 and C5ar1) G protein-coupled receptor signaling plays an obligate role in vascular endothelial growth factor receptor 2 growth signaling in vascular endothelial cells. We documented the same interconnection for platelet-derived growth factor receptor growth signaling in smooth muscle cells, epidermal growth factor receptor growth signaling in epidermal cells, and fibroblast growth factor receptor signaling in fibroblasts, indicative of a generalized cell growth regulatory mechanism...
February 19, 2024: Journal of Immunology
https://read.qxmd.com/read/38372637/role-for-caspase-8-in-the-release-of-il-1%C3%AE-and-active-caspase-1-from-viable-human-monocytes-during-toxoplasma-gondii-infection
#52
JOURNAL ARTICLE
William J Pandori, Stephanie Y Matsuno, Ji-Hun Shin, Samuel C Kim, Tiffany H Kao, Sharmila Mallya, Sarah N Batarseh, Melissa B Lodoen
Monocytes are actively recruited to sites of infection and produce the potent proinflammatory cytokine IL-1β. We previously showed that IL-1β release during Toxoplasma gondii infection of primary human monocytes requires the NLRP3 inflammasome and caspase-1 but is independent of gasdermin D and pyroptosis. To investigate mechanisms of IL-1β release, we generated caspase-1, -4, -5, or -8 knockout (KO) THP-1 monocytic cells. Genetic ablation of caspase-1 or -8, but not caspase-4 or -5, decreased IL-1β release during T...
February 19, 2024: Journal of Immunology
https://read.qxmd.com/read/38372634/molecular-interactions-required-for-activation-of-complement-component-c2-include-exosites-located-on-the-serine-protease-domain-of-c1s-and-mannose-binding-lectin-associated-protease-2
#53
JOURNAL ARTICLE
Lilian Hor, Jing Pan, Robert N Pike, Lakshmi C Wijeyewickrema
The activation of the CP/LP C3 proconvertase complex is a key event in complement activation and involves cleavage of C4 and C2 by the C1s protease (classical pathway) or the mannose-binding lectin-associated serine protease (MASP)-2 (lectin pathway). Efficient cleavage of C4 by C1s and MASP-2 involves exosites on the complement control protein and serine protease (SP) domains of the proteases. The complement control protein domain exosite is not involved in cleavage of C2 by the proteases, but the role of an anion-binding exosite (ABE) on the SP domains of the proteases has (to our knowledge) never been investigated...
February 19, 2024: Journal of Immunology
https://read.qxmd.com/read/38363226/cytotoxic-programming-of-cd4-t-cells-is-regulated-by-opposing-actions-of-the-related-transcription-factors-eos-and-aiolos
#54
JOURNAL ARTICLE
Devin M Jones, Jasmine A Tuazon, Kaitlin A Read, Melissa R Leonard, Srijana Pokhrel, Bharath K Sreekumar, Robert T Warren, Jacob S Yount, Patrick L Collins, Kenneth J Oestreich
In contrast to the "helper" activities of most CD4+ T effector subsets, CD4+ cytotoxic T lymphocytes (CD4-CTLs) perform functions normally associated with CD8+ T and NK cells. Specifically, CD4-CTLs secrete cytotoxic molecules and directly target and kill compromised cells in an MHC class II-restricted fashion. The functions of these cells have been described in diverse immunological contexts, including their ability to provide protection during antiviral and antitumor responses, as well as being implicated in autoimmunity...
February 16, 2024: Journal of Immunology
https://read.qxmd.com/read/38363205/cutting-edge-the-tetraspanin-cd53-promotes-cxcr4-signaling-and-bone-marrow-homing-in-b-cells
#55
JOURNAL ARTICLE
Mousumi Chakraborty, Zev J Greenberg, Qian Dong, Nate Roundy, Jeffrey J Bednarski, Luana Chiquetto Paracatu, Eric Duncavage, Weikai Li, Laura G Schuettpelz
B cell trafficking involves the coordinated activity of multiple adhesive and cytokine-receptor interactions, and the players in this process are not fully understood. In this study, we identified the tetraspanin CD53 as a critical regulator of both normal and malignant B cell trafficking. CXCL12 is a key chemokine in B cell homing to the bone marrow and secondary lymphoid organs, and both normal and malignant B cells from Cd53-/- mice have reduced migration toward CXCL12 in vitro, as well as impaired marrow homing in vivo...
February 16, 2024: Journal of Immunology
https://read.qxmd.com/read/38363204/fish-uses-ctla-4-immune-checkpoint-to-suppress-mtorc1-controlled-t-cell-glycolysis-and-immunity
#56
JOURNAL ARTICLE
Jiansong Zhang, Xiumei Wei, Qian Zhang, Xinying Jiao, Kang Li, Ming Geng, Yi Cao, Ding Wang, Jie Cheng, Jialong Yang
As an immune checkpoint, cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) suppresses the activation, proliferation, and effector function of T cells, thus preventing an overexuberant response and maintaining immune homeostasis. However, whether and how this immune checkpoint functions in early vertebrates remains unknown. In the current study, using a Nile tilapia (Oreochromis niloticus) model, we investigated the suppression of T cell response by CTLA-4 in bony fish. Tilapia CTLA-4 is constitutively expressed in lymphoid tissues, and its mRNA and protein expression in lymphocytes are upregulated following PHA stimulation or Edwardsiella piscicida infection...
February 16, 2024: Journal of Immunology
https://read.qxmd.com/read/38353647/cutting-edge-hypoxia-sensing-by-the-histone-demethylase-utx-kdm6a-limits-colitogenic-cd4-t-cells-in-mucosal-inflammation
#57
JOURNAL ARTICLE
Mandy I Cheng, Lee Hong, Christian Bustillos, Bryan Chen, Scott Chin, Christopher R Luthers, Au Vo, Shehzad Z Sheikh, Maureen A Su
Hypoxia is a hallmark of inflammatory conditions (e.g., inflammatory bowel disease [IBD]), and adaptive responses have consequently evolved to protect against hypoxia-associated tissue injury. Because augmenting hypoxia-induced protective responses is a promising therapeutic approach for IBD, a more complete understanding of these pathways is needed. Recent work has demonstrated that the histone demethylase UTX is oxygen-sensitive, but its role in IBD is unclear. In this study, we show that hypoxia-induced deactivation of UTX downregulates T cell responses in mucosal inflammation...
February 14, 2024: Journal of Immunology
https://read.qxmd.com/read/38353642/clec-1-restrains-acute-inflammatory-response-and-recruitment-of-neutrophils-following-tissue-injury
#58
JOURNAL ARTICLE
Camille Ligeron, Javier Saenz, Berangere Evrard, Marion Drouin, Emmanuel Merieau, Caroline Mary, Kevin Biteau, Emmanuelle Wilhelm, Cécile Batty, Vanessa Gauttier, Irene Baccelli, Nicolas Poirier, Elise Chiffoleau
The inflammatory response is a key mechanism for the elimination of injurious agents but must be tightly controlled to prevent additional tissue damage and progression to persistent inflammation. C-type lectin receptors expressed mostly by myeloid cells play a crucial role in the regulation of inflammation by recognizing molecular patterns released by injured tissues. We recently showed that the C-type lectin receptor CLEC-1 is able to recognize necrotic cells. However, its role in the acute inflammatory response following tissue damage had not yet been investigated...
February 14, 2024: Journal of Immunology
https://read.qxmd.com/read/38353615/failed-downregulation-of-pi3k-signaling-makes-autoreactive-b-cells-receptive-to-bystander-t-cell-help
#59
JOURNAL ARTICLE
Brigita E Fiske, Andrew Getahun
The role of T cell help in autoantibody responses is not well understood. Because tolerance mechanisms govern both T and B cell responses, one might predict that both T cell tolerance and B cell tolerance must be defeated in autoantibody responses requiring T cell help. To define whether autoreactive B cells depend on T cells to generate autoantibody responses, we studied the role of T cells in murine autoantibody responses resulting from acute B cell-specific deletion of regulatory phosphatases. Ars/A1 B cells are DNA reactive and require continuous inhibitory signaling by the tyrosine phosphatase SHP-1 and the inositol phosphatases SHIP-1 and PTEN to maintain unresponsiveness...
February 14, 2024: Journal of Immunology
https://read.qxmd.com/read/38353614/cutting-edge-phagosome-associated-autophagosomes-containing-antigens-and-proteasomes-drive-tap-independent-cross-presentation
#60
JOURNAL ARTICLE
Debrup Sengupta, Rodrigo Galicia-Pereyra, Patrick Han, Morven Graham, Xinran Liu, Najla Arshad, Peter Cresswell
Activation of naive CD8-positive T lymphocytes is mediated by dendritic cells that cross-present MHC class I (MHC-I)-associated peptides derived from exogenous Ags. The most accepted mechanism involves the translocation of Ags from phagosomes or endolysosomes into the cytosol, where antigenic peptides generated by cytosolic proteasomes are delivered by the transporter associated with Ag processing (TAP) to the endoplasmic reticulum, or an endocytic Ag-loading compartment, where binding to MHC-I occurs. We have described an alternative pathway where cross-presentation is independent of TAP but remains dependent on proteasomes...
February 14, 2024: Journal of Immunology
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